Clinical Trials Register

Summary
EudraCT Number:	2012-002714-40
Sponsor's Protocol Code Number:	RPC01-201
National Competent Authority:	Spain - AEMPS
Clinical Trial Type:	EEA CTA
Trial Status:	Completed
Date on which this record was first entered in the EudraCT database:	2013-04-09
Trial results	View results

Index
A. PROTOCOL INFORMATION
B. SPONSOR INFORMATION
C. APPLICANT IDENTIFICATION
D. IMP IDENTIFICATION
D.8 INFORMATION ON PLACEBO
E. GENERAL INFORMATION ON THE TRIAL
F. POPULATION OF TRIAL SUBJECTS
G. INVESTIGATOR NETWORKS TO BE INVOLVED IN THE TRIAL
N. REVIEW BY THE COMPETENT AUTHORITY OR ETHICS COMMITTEE IN THE COUNTRY CONCERNED
P. END OF TRIAL

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A. Protocol Information

A.1

Member State Concerned

Spain - AEMPS

A.2

EudraCT number

2012-002714-40

A.3

Full title of the trial

A PHASE 2/3, MULTI-CENTER, RANDOMIZED, DOUBLE-BLIND, PLACEBO CONTROLLED (PART A) AND DOUBLE-BLIND, DOUBLE-DUMMY, ACTIVE CONTROLLED (PART B), PARALLEL GROUP STUDY TO EVALUATE THE EFFICACY AND SAFETY OF RPC1063 ADMINISTERED ORALLY TO RELAPSING MULTIPLE SCLEROSIS PATIENTS

ESTUDIO FASE 2/3, MULTICÉNTRICO, ALEATORIZADO, DOBLE CIEGO, CONTROLADO CON PLACEBO (PARTE A) Y DOBLE CIEGO, CON DOBLE SIMULACIÓN Y CON CONTROL ACTIVO (PARTE B), DE GRUPOS PARALELOS PARA EVALUAR LA EFICACIA Y LA SEGURIDAD DE RPC1063 ADMINISTRADO POR VÍA ORAL A PACIENTES CON ESCLEROSIS MÚLTIPLE RECIDIVANTE

A.3.1

Title of the trial for lay people, in easily understood, i.e. non-technical, language

A CLINICAL STUDY TO EVALUATE IN A BLINDED AND SCIENTIFIC WAY THE EFFICACY AND SAFETY OF THE NEW MEDICINAL PRODUCT RPC1063 IN PATIENTS WITH RELAPSING MULTIPLE SCLEROSIS

Ensayo clínico para evaluar de una manera ciega y científica la eficacia y la seguridad del nuevo medicamento RPC1063 en pacientes con esclerosis múltiple recidivante

A.4.1

Sponsor's protocol code number

RPC01-201

A.5.2

US NCT (ClinicalTrials.gov registry) number

NCT01628393

A.7

Trial is part of a Paediatric Investigation Plan

A.8

EMA Decision number of Paediatric Investigation Plan

B. Sponsor Information
B.Sponsor: 1
B.1.1	Name of Sponsor	Receptos, Inc.
B.1.3.4	Country	United States
B.3.1 and B.3.2	Status of the sponsor	Commercial
B.4 Source(s) of Monetary or Material Support for the clinical trial:
B.4.1	Name of organisation providing support	Receptos, Inc.
B.4.2	Country	United States
B.5 Contact point designated by the sponsor for further information on the trial
B.5.1	Name of organisation	PPD
B.5.2	Functional name of contact point	Sabine Krofczik
B.5.3	Address:
B.5.3.1	Street Address	Hansastrasse 32
B.5.3.2	Town/ city	Munchen
B.5.3.3	Post code	80686
B.5.3.4	Country	Germany
B.5.4	Telephone number	4989380 38 298
B.5.5	Fax number	4989578 77 400
B.5.6	E-mail	sabine.krofczik@ppdi.com

D. IMP Identification
D.IMP: 1
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	No
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	0.25 mg RPC1063
D.3.4	Pharmaceutical form	Capsule
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Oral use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	RPC1063
D.3.9.2	Current sponsor code	RPC1063
D.3.10	Strength
D.3.10.1	Concentration unit	mg milligram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	0.25
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	Yes
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 2
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	No
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	0.5 mg RPC1063
D.3.4	Pharmaceutical form	Capsule
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Oral use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	RPC1063
D.3.9.2	Current sponsor code	RPC1063
D.3.10	Strength
D.3.10.1	Concentration unit	mg milligram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	0.50
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	Yes
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 3
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	No
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	1 mg RPC1063
D.3.4	Pharmaceutical form	Capsule
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Oral use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	RPC1063
D.3.9.2	Current sponsor code	RPC1063
D.3.10	Strength
D.3.10.1	Concentration unit	mg milligram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	1
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	Yes
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 4
D.1.2 and D.1.3	IMP Role	Comparator
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	Yes
D.2.1.1.1	Trade name	Avonex
D.2.1.1.2	Name of the Marketing Authorisation holder	Biogen Idec Limited
D.2.1.2	Country which granted the Marketing Authorisation	Spain
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	Avonex
D.3.4	Pharmaceutical form	Solution for injection
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intramuscular use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	Avonex
D.3.9.1	CAS number	220581-49-7
D.3.9.3	Other descriptive name	INTERFERON BETA-1A
D.3.9.4	EV Substance Code	SUB12440MIG
D.3.10	Strength
D.3.10.1	Concentration unit	µg microgram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	30
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	No
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	Yes
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	Yes
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No

D.8 Information on Placebo
D.8 Placebo: 1
D.8.1	Is a Placebo used in this Trial?	Yes
D.8.3	Pharmaceutical form of the placebo	Capsule
D.8.4	Route of administration of the placebo	Oral use
D.8 Placebo: 2
D.8.1	Is a Placebo used in this Trial?	Yes
D.8.3	Pharmaceutical form of the placebo	Solution for injection
D.8.4	Route of administration of the placebo	Intramuscular use

E. General Information on the Trial

E.1 Medical condition or disease under investigation

E.1.1

Medical condition(s) being investigated

RELAPSING MULTIPLE SCLEROSIS

ESCLEROSIS MÚLTIPLE RECIDIVANTE

E.1.1.1

Medical condition in easily understood language

RELAPSING MULTIPLE SCLEROSIS

ESCLEROSIS MÚLTIPLE RECIDIVANTE

E.1.1.2

Therapeutic area

Diseases [C] - Nervous System Diseases [C10]

MedDRA Classification

E.1.2 Medical condition or disease under investigation

E.1.2	Version	14.1
E.1.2	Level	PT
E.1.2	Classification code	10048393
E.1.2	Term	Multiple sclerosis relapse
E.1.2	System Organ Class	10029205 - Nervous system disorders

E.1.3

Condition being studied is a rare disease

E.2 Objective of the trial

E.2.1

Main objective of the trial

Part A
To demonstrate the superior clinical efficacy of RPC1063 compared to placebo by showing a reduction in the cumulative number of total gadolinium enhancing (GdE) lesions from Week 12 to Week 24 in patients with relapsing multiple sclerosis (RMS).
Part B
To assess whether the clinical efficacy of RPC1063 is superior to interferon (IFN) Beta-1a (Avonex®) in reducing the rate of clinical relapses at the end of Month 24 in patients with RMS.

Parte A
Demostrar la eficacia clínica superior de RPC1063 con respecto a placebo mediante la constatación de una reducción del número acumulado de lesiones totales con captación de gadolinio (CGd) entre las semanas 12 y 24 en pacientes con esclerosis múltiple recidivante (EMR).
Parte B
Evaluar si la eficacia clínica de RPC1063 es superior a la del interferón (IFN) Beta-1a (Avonex®) en lo que respecta a reducir la tasa de recidivas clínicas al final del mes 24 en pacientes con EMR.

E.2.2

Secondary objectives of the trial

Part A
- assess the proportion of patients who are free of GdE lesions at Week 24
-assess the effect of RPC1063 on the cumulative number of new/enlarging T2 lesions from W12 to W24
-compare the clinical efficacy of RPC1063 to placebo in pts with RMS by reduction in ARR & proportion of relapse free pts at W24
-assess the safety, tolerability, PK and PD of RPC1063 in pts with RMS
Part B
-assess the effect of RPC1063 on the proportion of patients with new/enlarging T2 lesions at M24
-evaluate whether the efficacy of RPC1063 is superior to IFN Beta-1a in delaying the accumulation of disability, measured by MSFC and by the SLCLA
-evaluate whether the efficacy of RPC1063 is superior to IFN Beta-1a in delaying the accumulation of disability, as assessed by the EDSS
-assess the effect of RPC1063 on brain atrophy over 24m
-evaluate the effect of RPC1063 on patient-reported quality of life as assessed by the MSQOL-54
-assess the safety & tolerability of RPC1063 in pts with RMS

Parte A
- Evaluar proporción de pacientes sin lesiones con CGd en la semana (Sem.) 24
- Evaluar efecto de RPC1063 sobre el nº. acumulado de lesiones en T2 nuevas o que aumenten de tamaño entre las Sem. 12 y 24
- Comparar eficacia clínica de RPC1063 con placebo en pacientes con EMR
- Evaluar seguridad, tolerabilidad, FC y FD de RPC1063 en pacientes con EMR
Parte B
- Evaluar efecto de RPC1063 sobre la proporción de pacientes con lesiones en T2 nuevas o que aumenten de tamaño en el mes 24
- Evaluar si la eficacia de RPC1063 es superior a la de IFN B-1a en retrasar la acumulación de discapacidad
- Evaluar si la eficacia de RPC1063 es superior a la de IFN B-1a en retrasar la acumulación de discapacidad
- Evaluar el efecto de RPC1063 sobre la atrofia cerebral durante 24 meses
- Evaluar el efecto de RPC1063 sobre la calidad de vida comunicada por el paciente
- Evaluar la seguridad y la tolerabilidad de RPC1063 en pacientes con EMR

E.2.3

Trial contains a sub-study

E.3

Principal inclusion criteria

Per Protocol dated 14 September 2012.

1.MS, as diagnosed by the revised 2010 McDonald criteria
2.Exhibiting a relapsing clinical course consistent with RMS and history of brain MRI lesions consistent with MS
3.Ages 18-55 years, inclusive
4.EDSS score between 0 and 5.0 at baseline
5.Meet one of the following disease activity criteria:
a.At least 1 documented relapse within the last 12 months prior to screening
OR
b.At least 1 documented relapse occurred within the last 24 months prior to screening and documented evidence of at least 1 GdE lesion on brain MRI within the last 12 months prior to randomization
6.No history of relapse with onset from 30 days prior to screening until randomization; during this period, patients must have been clinically stable, without systemic corticosteroid treatment or adrenocorticotrophic hormone (ACTH)
7.Ability to provide written informed consent and to be compliant with the schedule of protocol assessments
8.Patients of reproduction potential (males and females) must practice an acceptable method of birth control (acceptable methods of birth control in this study include: surgical sterilization, intrauterine devices, oral contraceptive, contraceptive patch, long acting injectable contraceptive, vasectomy or double-barrier method [condom or diaphragm with spermicide]) during study participation and for 30 days after their last dose of treatment of study medication or abstinence
9.Documentation of positive Varicella Zoster virus (VZV) IgG antibody status

Según el protocolo de fecha 14 de septiembre de 2012

1. EM, diagnosticada mediante los criterios revisados de McDonald de 2010.
2. Presencia de una evolución clínica recidivante compatible con EMR y antecedentes de lesiones en la RM cerebral compatibles con EM.
3. Edad de 18-55 años, ambos inclusive.
4. Puntuación EDSS de entre 0 y 5,0 en el momento basal.
5. Cumplimiento de uno de los siguientes criterios de actividad de la enfermedad:
a. Al menos una recidiva documentada en los 12 meses previos a la selección.
O BIEN
b. Al menos una recidiva documentada en los 24 meses previos a la selección y datos documentados de al menos una lesión con CGd en la RM cerebral en los 12 meses previos a la aleatorización.
6. Ausencia de antecedentes de recidivas con comienzo entre 30 días antes de la selección y la aleatorización; durante este período, los pacientes deberán haber permanecido clínicamente estables, sin tratamiento con corticosteroides sistémicos ni corticotropina (ACTH).
7. Capacidad de otorgar el consentimiento informado por escrito y de cumplir el calendario de evaluaciones del protocolo.
8. Los pacientes con capacidad reproductiva (varones y mujeres) deberán utilizar un método anticonceptivo aceptable (los métodos anticonceptivos aceptables en este estudio comprenden: esterilización quirúrgica, dispositivos intrauterinos, anticonceptivos orales, parches anticonceptivos, anticonceptivos inyectables de acción prolongada, vasectomía o método de doble barrera [preservativo o diafragma con espermicida]) durante la participación en el estudio y durante 30 días después de la última dosis del tratamiento del estudio o abstinencia.
9. Documentación de la presencia de anticuerpos IgG contra el virus de la varicela-zóster (VVZ).

E.4

Principal exclusion criteria

Per Protocol dated 14 September 2012.

1.Primary progressive MS at screening
2.Disease duration of more than 15 years in patients with an EDSS <= 2.0
3.Contraindications to MRI or Gadolinium contrast, including known allergy to Gadolinium contrast dyes, renal insufficiency, claustrophobia, weight >= 300 lb (>= 136 kg), pacemaker, cochlear implants, intracranial vascular clips
4.Incompatibility with beta IFN use (e.g. intolerable side effects) (Part B only)
Exclusions Related to General Health:
5.Pregnancy, lactation, or a positive serum beta human chorionic gonadotrophin (hCG) measured during screening
6.Clinically relevant hepatic, neurological, pulmonary, ophthalmological, endocrine, renal, or other major systemic disease making implementation of the protocol or interpretation of the study results difficult or that would put the patient at risk by participating in the study in the opinion of treating investigator
7.Clinically relevant cardiovascular conditions, including history or presence of ischemic heart disease, myocardial infarction, congestive heart failure, stroke, transient ischemic attack, sick sinus syndrome, recurrent syncope, second degree or higher AV block, prolonged QTcF interval (QTcF > 450 msec males, > 470 msec females), other clinically significant conduction abnormalities or any other significant cardiac condition that could jeopardize a patient?s health during the course of the study in the opinion of treating investigator
8.Resting heart rate less than 55 bpm
9.History of diabetes mellitus
10.History of uveitis
11.Known active bacterial, viral, fungal, mycobacterial infection, or other infection (including tuberculosis [TB] or atypical mycobacterial disease [but excluding fungal infection of nail beds]) or any major episode of infection that required hospitalization or treatment with IV antibiotics within 30 days of screening or oral antibiotics within 14 days prior to screening
12.History or known presence of recurrent or chronic infection (e.g., hepatitis A, B, C, or E, human immunodeficiency virus (HIV), syphilis, TB); recurring urinary tract infections could be allowed
13.History of cancer, including solid tumors and hematological malignancies (except basal cell and in situ squamous cell carcinomas of the skin that have been excised and resolved)
14.Suicide attempts in the past or current signs of major depression
15.History of alcohol or drug abuse within 1 year prior to randomization
16.History of or currently active primary or secondary immunodeficiency
Exclusions Related to Medications:
17.Prior use of any investigational agent within 6 months prior to enrollment
18.Receipt of a live vaccine within 4 weeks prior to screening
19.Non-lymphocyte-depleting disease-modifying MS agents (e.g., glatiramer acetate, interferons) must be discontinued from signing of informed consent until randomization
20.Previous treatment with lymphocyte-depleting therapies (e.g., alemtuzumab, anti-CD4, cladribine, rituximab, ocrelizumab, cyclophosphamide, mitoxantrone, total body irradiation, bone marrow transplantation)
21.Treatment with other immunosuppressant agents such as azathioprine, cyclosporine, methotrexate, or mycophenolate within 6 months prior to randomization
22.Systemic corticosteroid therapy or ACTH use within 30 days prior to screening.
23.Prior treatment with lymphocyte trafficking blockers (e.g., natalizumab, fingolimod, other S1PR agonists).
24.Treatment with intravenous immune globulin (IVIg), plasmapheresis, within 3 months prior to randomization
25.Previous treatment with any monoclonal antibody
26.Intolerance of or contraindication to oral or IV corticosteroids
27.Use of therapies that are not allowed based on CYP3A4 metabolism within 4 weeks prior to randomization
28.Treatment with medications with a known impact on the cardiac conduction system (e.g., beta blockers, calcium channel blockers, Class Ia or Class III anti-arrhythmic drugs)
Exclusions Related to Laboratory Results:
29.Vitamin B12 below the lower limit of normal
30.Positive rapid plasma reagin
31.Serum creatinine > 1.4 mg/dL for women or > 1.6 mg/dL for men
32.Liver function impairment or persisting elevations of aspartate aminotransferase (SGOT/AST) or alanine aminotransferase (SGPT/ALT) > 1.5 times the upper limit of normal (ULN), or direct bilirubin > 1.5 times the ULN
33.Platelet count < 100,000/mcL
34.Hemoglobin < 8.5 g/dL
35.Neutrophils < 1.5/mcL
36.Absolute white blood cell (WBC) count < 3500/mcL; absolute lymphocyte count < 800/mcL
37.Clinically significant findings on brain MRI scan consistent with conditions other than MS
38.ECG showing any clinically significant abnormality (e.g., acute ischemia, significant heart conduction abnormality (e.g. left bundle branch block))
39.FEV1 and FVC < 70% of predicted values at screening
40.Presence of > 20 gadolinium-enhancing lesions on baseline brain MRI scan

Según el protocolo de fecha 14 de septiembre de 2012

1. EM progresiva primaria en el momento de selección.
2. Duración de la enfermedad superior a 15 años en pacientes con una puntuación EDSS <= 2,0.
3. Contraindicaciones de la RM o el contraste con gadolinio, entre ellas, alergia conocida a los medios de contraste con gadolinio, insuficiencia renal, claustrofobia, peso >= 136 kg, marcapasos, implantes cocleares o clips intracraneales vasculares.
4. Incompatibilidad con el uso de IFN-beta (por ejemplo, efectos secundarios intolerables) (solo parte B).
Exclusiones relacionadas con el estado de salud general:
5. Embarazo, lactancia o beta-gonadotropina coriónica humana (hCG) en suero positiva medida durante la selección.
6. Enfermedad hepática, neurológica, respiratoria, oftalmológica, endocrina, renal u otra enfermedad sistémica grave clínicamente relevante que dificulte la aplicación del protocolo o la interpretación de los resultados del estudio o que pueda poner en peligro al paciente por participar en el estudio.
7. Enfermedades cardiovasculares clínicamente relevantes, como antecedentes o presencia de cardiopatía isquémica, infarto de miocardio, insuficiencia cardíaca congestiva, ictus, accidente isquémico transitorio, síndrome del seno enfermo, síncope recurrente, bloqueo AV de segundo grado o superior, prolongación del intervalo QTcF, otras anomalías de la conducción clínicamente significativas o cualquier otra cardiopatía importante que pueda poner en peligro la salud del paciente durante el transcurso del estudio.
8. Frecuencia cardíaca en reposo inferior a 55 lpm.
9. Antecedentes de diabetes mellitus.
10. Antecedentes de uveítis.
11. Infección bacteriana, vírica, micótica, micobacteriana o de otro tipo activa conocida o cualquier episodio grave de infección con necesidad de hospitalización o tratamiento con antibióticos IV en los 30 días previos a la selección o con antibióticos orales en los 14 días previos a la selección.
12. Antecedentes o presencia conocida de una infección recurrente o crónica; podría permitirse la existencia de infecciones urinarias recurrentes.
13. Antecedentes de cáncer, incluidos tumores sólidos y neoplasias hematológicas malignas.
14. Intentos de suicidio en el pasado o signos presentes de depresión mayor.
15. Antecedentes de alcoholismo o toxicomanía en el año previo a la aleatorización.
16. Antecedentes o presencia activa de una inmunodeficiencia primaria o secundaria.
Exclusiones relacionadas con medicamentos:
17. Uso previo de cualquier fármaco en investigación en los 6 meses previos al reclutamiento.
18. Vacunación con una vacuna de microorganismos vivos en las 4 semanas previas a la selección.
19. Los fármacos para la EM que sean modificadores de la enfermedad, pero sin reducir los linfocitos, deberán suspenderse desde la firma del consentimiento informado y hasta la aleatorización.
20. Tratamiento previo con terapias que reduzcan los linfocitos.
21. Tratamiento con otros inmunodepresores como azatioprina, ciclosporina, metotrexato o micofenolato mofetilo en los 6 meses previos a la aleatorización.
22. Tratamiento con corticosteroides sistémicos o uso de ACTH en los 30 días previos a la selección.
23. Tratamiento previo con bloqueantes del tráfico de linfocitos.
24. Tratamiento con inmunoglobulina intravenosa (IgIV) o plasmaféresis en los 3 meses previos a la aleatorización.
25. Tratamiento previo con cualquier anticuerpo monoclonal.
26. Intolerancia o contraindicación a los corticosteroides por vía oral o IV.
27. Uso de tratamientos prohibidos en función del metabolismo por CYP3A4 en las 4 semanas previas a la aleatorización.
28. Tratamiento con medicamentos con efectos conocidos sobre el sistema de conducción cardíaco (por ejemplo, betabloqueantes, antagonistas del calcio o antiarrítmicos de clase Ia o III).
Exclusiones relacionadas con resultados analíticos:
29. Vitamina B12 por debajo del límite inferior de la normalidad.
30. Resultado positivo para reagina plasmática rápida.
31. Creatinina sérica > 1,4 mg/dl en las mujeres o > 1,6 mg/dl en los varones.
32. Insuficiencia hepática o elevaciones persistentes de la aspartato aminotransferasa (SGOT/AST) o alanina aminotransferasa (SGPT/ALT) > 1,5 veces el límite superior de la normalidad (LSN) o bilirrubina directa > 1,5 veces el LSN.
33. Recuento de plaquetas < 100.000/microl.
34. Hemoglobina < 8,5 g/dl.
35. Neutrófilos < 1,5/microl.
36. Recuento absoluto de leucocitos < 3500/microl; recuento absoluto de linfocitos < 800/microl.
37. Hallazgos clínicamente significativos en la RM cerebral compatibles con enfermedades distintas de la EM.
38. ECG con anomalías clínicamente significativas (por ejemplo, isquemia aguda o alteración significativa de la conducción cardíaca (por ejemplo, bloqueo de rama izquierda)).
39. FEV1 y FVC < 70 % de los valores teóricos en el momento de selección.
40. Presencia de más de 20 lesiones con captación de gadolinio en la RM cerebral basal.

E.5 End points

E.5.1

Primary end point(s)

Primary Efficacy Endpoint:
Part A: Total number of GdE lesions, assessed on brain MRIs from Week 12 to Week 24
Part B: ARR at the end of Month 24

Criterio de valoración principal de la eficacia:
Parte A: número total de lesiones con CGd, evaluadas en la RM cerebral entre las semanas 12 y 24.
Parte B: TAR al final del mes 24.

E.5.1.1

Timepoint(s) of evaluation of this end point

Please see section E.5.1 above

Refiéranse a la sección E.5.1 de arriba

E.5.2

Secondary end point(s)

Secondary Efficacy Endpoints:
Part A:
Key Secondary Endpoints (rank ordered):
- The number of GdE lesions at Week 24
- Total number of new or enlarging hyperintense T2-weighted brain MRI lesions from Week 12 to Week 24
- ARR at the end of Week 24
Part B:
Key Secondary Endpoints (rank ordered):
- The number of new or enlarging hyperintense T2-weighted brain MRI lesions at Month 24
- Change in MSFC score and visual function as measured by the SLCLA
- Time to onset of sustained disability progression as defined by a sustained worsening in EDSS of 1.0 points or more, confirmed after 12 weeks
- Time to onset of sustained disability progression as defined by a sustained worsening in EDSS of 1.0 points or more, confirmed after 24 weeks
- The change in brain atrophy on brain MRI scans from baseline to 24 months
- Change in MSQOL-54 score at 24 months

Criterios de valoración secundarios de la eficacia:
Parte A:
Criterios de valoración secundarios fundamentales (ordenados por rango):
- Número de lesiones con CGd en la semana 24.
- Número total de lesiones hiperintensas en T2 nuevas o que aumenten de tamaño en la RM cerebral entre las semanas 12 y 24.
- TAR al final de la semana 24.
Parte B:
Criterios de valoración secundarios fundamentales (ordenados por rango):
- Número de lesiones hiperintensas en T2 nuevas o que aumenten de tamaño en la RM cerebral en el mes 24.
- Variación de la puntuación MSFC y la función visual medida mediante la prueba SLCLA.
- Tiempo hasta la aparición de progresión mantenida de la discapacidad, definida como un empeoramiento mantenido de la puntuación EDSS de 1,0 puntos o más, confirmado después de 12 semanas.
- Tiempo hasta la aparición de progresión mantenida de la discapacidad, definida como un empeoramiento mantenido de la puntuación EDSS de 1,0 puntos o más, confirmado después de 24 semanas.
- Variación de la atrofia cerebral en la RM cerebral entre el momento basal y el mes 24.
- Variación de la puntuación MSQOL-54 a los 24 meses.

E.5.2.1

Timepoint(s) of evaluation of this end point

Please see section E.5.2 above

Refiéranse a la sección E.5.2 de arriba

E.6 and E.7 Scope of the trial

E.6

Scope of the trial

E.6.1

Diagnosis

E.6.2

Prophylaxis

E.6.3

Therapy

Yes

E.6.4

Safety

Yes

E.6.5

Efficacy

Yes

E.6.6

Pharmacokinetic

Yes

E.6.7

Pharmacodynamic

Yes

E.6.8

Bioequivalence

E.6.9

Dose response

E.6.10

Pharmacogenetic

E.6.11

Pharmacogenomic

E.6.12

Pharmacoeconomic

E.6.13

Others

E.7

Trial type and phase

E.7.1

Human pharmacology (Phase I)

E.7.1.1

First administration to humans

E.7.1.2

Bioequivalence study

E.7.1.3

Other

E.7.1.3.1

Other trial type description

E.7.2

Therapeutic exploratory (Phase II)

Yes

E.7.3

Therapeutic confirmatory (Phase III)

Yes

E.7.4

Therapeutic use (Phase IV)

E.8 Design of the trial

E.8.1

Controlled

Yes

E.8.1.1

Randomised

Yes

E.8.1.2

Open

E.8.1.3

Single blind

E.8.1.4

Double blind

Yes

E.8.1.5

Parallel group

Yes

E.8.1.6

Cross over

E.8.1.7

Other

Yes

E.8.1.7.1

Other trial design description

Doble simulación

Double-Dummy

E.8.2

Comparator of controlled trial

E.8.2.1

Other medicinal product(s)

Yes

E.8.2.2

Placebo

Yes

E.8.2.3

Other

E.8.2.4

Number of treatment arms in the trial

E.8.3

The trial involves single site in the Member State concerned

E.8.4

The trial involves multiple sites in the Member State concerned

Yes

E.8.4.1

Number of sites anticipated in Member State concerned

E.8.5

The trial involves multiple Member States

Yes

E.8.5.1

Number of sites anticipated in the EEA

E.8.6 Trial involving sites outside the EEA

E.8.6.1

Trial being conducted both within and outside the EEA

Yes

E.8.6.2

Trial being conducted completely outside of the EEA

E.8.6.3

If E.8.6.1 or E.8.6.2 are Yes, specify the regions in which trial sites are planned

Belgium

Bulgaria

Canada

Czech Republic

Georgia

Greece

Hungary

Israel

Italy

Poland

Romania

Russian Federation

Serbia

Spain

Sweden

Ukraine

United Kingdom

United States

E.8.7

Trial has a data monitoring committee

Yes

E.8.8

Definition of the end of the trial and justification where it is not the last visit of the last subject undergoing the trial

LVLS

UVUP

E.8.9 Initial estimate of the duration of the trial

E.8.9.1

In the Member State concerned years

E.8.9.1

In the Member State concerned months

E.8.9.1

In the Member State concerned days

E.8.9.2

In all countries concerned by the trial years

E.8.9.2

In all countries concerned by the trial months

E.8.9.2

In all countries concerned by the trial days

F. Population of Trial Subjects

F.1 Age Range

F.1.1

Trial has subjects under 18

F.1.1.1

In Utero

F.1.1.2

Preterm newborn infants (up to gestational age < 37 weeks)

F.1.1.3

Newborns (0-27 days)

F.1.1.4

Infants and toddlers (28 days-23 months)

F.1.1.5

Children (2-11years)

F.1.1.6

Adolescents (12-17 years)

F.1.2

Adults (18-64 years)

Yes

F.1.2.1

Number of subjects for this age range:

1280

F.1.3

Elderly (>=65 years)

F.1.3.1

Number of subjects for this age range:

F.2 Gender

F.2.1

Female

Yes

F.2.2

Male

Yes

F.3 Group of trial subjects

F.3.1

Healthy volunteers

F.3.2

Patients

Yes

F.3.3

Specific vulnerable populations

Yes

F.3.3.1

Women of childbearing potential not using contraception

F.3.3.2

Women of child-bearing potential using contraception

Yes

F.3.3.3

Pregnant women

F.3.3.4

Nursing women

F.3.3.5

Emergency situation

F.3.3.6

Subjects incapable of giving consent personally

F.3.3.7

Others

F.4 Planned number of subjects to be included

F.4.1

In the member state

F.4.2

For a multinational trial

F.4.2.1

In the EEA

596

F.4.2.2

In the whole clinical trial

1280

F.5

Plans for treatment or care after the subject has ended the participation in the trial (if it is different from the expected normal treatment of that condition)

Standard of care

Cuidado habitual

G. Investigator Networks to be involved in the Trial

N. Review by the Competent Authority or Ethics Committee in the country concerned

Competent Authority Decision

Authorised

Date of Competent Authority Decision

2013-08-02

Ethics Committee Opinion of the trial application

Favourable

Ethics Committee Opinion: Reason(s) for unfavourable opinion

Date of Ethics Committee Opinion

2013-05-07

P. End of Trial
P.	End of Trial Status	Completed
P.	Date of the global end of the trial	2017-04-13

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Orphan Designation Number:
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